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首页> 外文期刊>Journal of Cerebral Blood Flow and Metabolism: Official Journal of the International Society of Cerebral Blood Flow and Metabolism >Effect of JTP-2942, a novel thyrotropin-releasing hormone analog, on motor deficits after chronic focal cerebral ischemia in rats.
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Effect of JTP-2942, a novel thyrotropin-releasing hormone analog, on motor deficits after chronic focal cerebral ischemia in rats.

机译:新型促甲状腺激素释放激素类似物JTP-2942对大鼠慢性局灶性脑缺血后运动功能障碍的影响。

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摘要

To investigate the chronic effects of a novel thyrotropin-releasing hormone analog, JTP-2942 (N(alpha)-[(1S, 2R)-2-methyl-4-oxocyclopentylcarbonyl]-L-histidyl-L-prolinamide monohydrate), on behavioral changes after stroke, the authors examined its effects on motor and neurologic deficits using a middle cerebral artery (MCA) occlusion model in rats. A left MCA was permanently occluded at a proximal site. From 1 week after occlusion, JTP-2942 was intravenously administered once a day for 4 weeks. Sensorimotor performance was evaluated weekly for 10 weeks after the occlusion. The ability of the rat to maintain its body position on an inclined plane and neurologic examination based on hemiparesis and abnormal posture were examined. After all behavioral examinations were completed, the degree of shrinkage of the left hemisphere was measured. The ability of MCA-occluded rats to maintain body position on an inclined plane in the left-headed position was significantly lower than that of sham-operated rats throughout the test period. JTP-2942 gradually improved this deficit dose dependently, and a dose of 0.03 mg/kg of JTP-2942 significantly improved performance to the levels of the sham-operated rats. Neurologic deficits were also observed in MCA-occluded rats. JTP-2942 also significantly improved these deficits dose dependently. On the other hand, CDP-choline (500 mg/kg, administered intravenously), a therapeutic agent for the disturbance of consciousness and hemiparesis after stroke, improved neurologic deficits but did not affect the motor deficits measured using the inclined plane. It is noteworthy that the effects of JTP-2942 on these deficits were observed 4 weeks after cessation of drug administration. Furthermore, there was no difference in the degree of shrinkage of the cerebrum among the MCA-occluded groups. In the present study, long-lasting improving effects of JTP-2942 on the impairment of motor and neurologic functions were observed in rats with MCA occlusion, which continued after cessation of drug administration and which were not attributable to a reduction in ipsilateral cerebral shrinkage. It is considered that the effect of JTP-2942 on functional recovery is attributable to the activation of substitutive functions such as neuronal reconstruction. These pharmacologic properties of JTP-2942 may be of interest for the treatment of patients with motor and neurologic deficits during the chronic or subacute phase of stroke.
机译:为了研究新型促甲状腺激素释放激素类似物JTP-2942(Nα-[(1S,2R)-2-甲基-4-氧代环戊基羰基] -L-组氨酸-L-脯氨酰胺一水合物)的慢性影响,中风后行为改变,作者使用大脑中动脉(MCA)闭塞模型检查了其对运动和神经功能缺损的影响。左MCA永久性阻塞在近端部位。从闭塞后1周开始,JTP-2942每天静脉注射一次,持续4周。闭塞后10周每周评估一次感觉运动表现。检查了大鼠在倾斜平面上保持身体姿势的能力以及基于偏瘫和异常姿势的神经系统检查。完成所有行为检查后,测量左半球的收缩程度。在整个测试期间,被MCA封堵的大鼠将身体位置保持在左头斜面上的能力明显低于假手术的大鼠。 JTP-2942逐渐逐渐改善了这种赤字剂量,0.03 mg / kg的JTP-2942剂量显着提高了假手术大鼠的水平。在MCA阻塞的大鼠中也观察到神经功能缺损。 JTP-2942还可以显着改善剂量依赖性的这些赤字。另一方面,CDP-胆碱(500 mg / kg,静脉给药)是中风后意识障碍和偏瘫的治疗剂,可改善神经功能缺损,但不影响使用斜面测量的运动功能障碍。值得注意的是,在停止给药后4周,观察到JTP-2942对这些缺陷的作用。此外,在MCA封闭组中,大脑的收缩程度没有差异。在本研究中,在MCA闭塞大鼠中观察到JTP-2942对运动和神经功能损害的持久改善作用,在停止给药后这种作用持续存在,并且不归因于同侧脑萎缩的减少。认为JTP-2942对功能恢复的作用归因于替代功能的激活,例如神经元重建。 JTP-2942的这些药理特性对于中风的慢性或亚急性期运动和神经功能缺损的患者的治疗可能感兴趣。

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